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Circadian Control of Metabolism

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Circadian Basics - Tick-Tock Metabolic Beat

  • Master Clock: Suprachiasmatic Nucleus (SCN) in hypothalamus; light-entrained.
  • Core Clock Genes (TTFL):
    • Activators: CLOCK, BMAL1 (form heterodimer).
    • Bind E-box elements → transcribe PER, CRY.
    • Repressors: PER, CRY proteins inhibit CLOCK/BMAL1.
    • Cycle duration: ~24 hours.
  • Metabolic Integration: SCN synchronizes peripheral clocks (liver, pancreas, adipose) for rhythmic metabolism (glucose, lipids).

⭐ Chronic circadian disruption (e.g., shift work) significantly elevates risk for metabolic syndrome and type 2 diabetes.

Peripheral Clocks - Metabolic Mini-Me's

  • SCN synchronizes peripheral clocks in key metabolic organs: liver, pancreas, adipose tissue, and muscle.
  • Communication occurs via neural (autonomic nervous system) and hormonal signals (e.g., glucocorticoids, melatonin).
  • These organ-specific clocks regulate local metabolic functions:
    • Liver: Controls glucose homeostasis, lipid metabolism, detoxification.
    • Pancreas: Manages rhythmic insulin and glucagon secretion.
    • Adipose Tissue: Regulates lipogenesis, adipokine release (e.g., leptin).
    • Muscle: Influences glucose uptake, energy expenditure.
  • Food intake is a primary zeitgeber (synchronizer) for peripheral clocks, especially for the liver. Circadian Control of Metabolism

⭐ Restricted feeding schedules can uncouple peripheral clocks (e.g., in the liver) from the SCN, demonstrating food's potent, independent influence on metabolic rhythmicity an exam-favourite concept for understanding shift work effects on metabolism.

Hormonal Rhythms - Rhythmic Regulators

  • Circadian clock orchestrates metabolic hormone release, aligning physiology with day-night cycles.
  • Key hormones exhibit distinct rhythmic secretion patterns impacting glucose homeostasis and energy balance.
HormonePeak SecretionKey Metabolic Actions
CortisolEarly Morning (Wake-up)↑Gluconeogenesis, ↑Insulin resistance, ↑Lipolysis
InsulinPost-prandial (Meal times)↑Glucose uptake & storage, ↑Lipogenesis, ↓Gluconeogenesis
GlucagonFasting (e.g., night)↑Glycogenolysis, ↑Gluconeogenesis
LeptinNight (During sleep)↓Appetite, ↑Energy expenditure
GhrelinPre-prandial, Night↑Appetite, ↑GH secretion, ↑Fat storage

⭐ Ghrelin, the "hunger hormone," typically peaks before meals and during the night, stimulating appetite.

Macronutrient Rhythms - Fueling by the Clock

Macronutrient (carb, lipid, protein) metabolism follows distinct daily rhythms, crucial for energy balance.

  • Carbohydrates:
    • Glucose tolerance & insulin sensitivity: ↑ AM (morning peak), ↓ PM (evening decline).
    • Pancreatic β-cell insulin secretion peaks during the body's active phase.
  • Lipids:
    • Lipogenesis (fat storage): ↑ with feeding, mainly during the active phase.
    • Lipolysis (fat breakdown): ↑ during fasting, predominantly in the inactive phase.
  • Proteins:
    • Synthesis & breakdown are linked to feeding-fasting cycles and physical activity patterns.
  • Digestion & Absorption:
    • Rhythmic secretion of digestive enzymes (amylase, lipase).
    • Nutrient transporter (e.g., SGLT1) expression varies, impacting uptake.

⭐ Insulin sensitivity is generally highest in the morning, promoting efficient glucose utilization. Circadian Rhythms and Metabolic Health

Clinical Impact - When Timing Goes Wrong

  • Circadian disruption (e.g., shift work, jet lag, irregular eating) impairs metabolic health.
  • Leads to: ↑ obesity, Type 2 Diabetes (T2DM), metabolic syndrome.
  • Shift work: associated with altered appetite hormones (↑ ghrelin, ↓ leptin), insulin resistance.
  • Chrononutrition: synchronizing meals with internal body clocks.
  • Time-Restricted Feeding (TRF): confining eating to specific daily windows (e.g., 8-12 hours) as a potential intervention.

    ⭐ Chronic circadian misalignment, as seen in night shift workers, significantly increases the risk of developing T2DM and cardiovascular diseases.

High‑Yield Points - ⚡ Biggest Takeaways

  • SCN is the master clock, synchronizing peripheral clocks in metabolic organs.
  • Peripheral clocks (liver, pancreas, adipose) directly regulate metabolic genes.
  • Clock genes (e.g., CLOCK, BMAL1, PER, CRY) form transcriptional-translational feedback loops.
  • Circadian misalignment (e.g., shift work) ↑ risk of obesity, type 2 diabetes, and cardiovascular disease.
  • Feeding-fasting cycles are major zeitgebers for peripheral metabolic clocks.
  • Key hormones like insulin, glucagon, and cortisol exhibit circadian rhythmicity, influencing metabolism.
  • Melatonin also plays a role in glucose homeostasis and energy balance regulation.

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